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10.1080/07391102.2020.1818626

http://scihub22266oqcxt.onion/10.1080/07391102.2020.1818626
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suck abstract from ncbi

pmid32909925      J+Biomol+Struct+Dyn 2022 ; 40 (2): 752-763
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  • Exploring structural dynamics of the MERS-CoV receptor DPP4 and mutant DPP4 receptors #MMPMID32909925
  • Alaofi AL
  • J Biomol Struct Dyn 2022[Feb]; 40 (2): 752-763 PMID32909925show ga
  • Mouse DPP4 (mDPP4) receptor is not a functional receptor for MERS-CoV while human DPP4 (hDPP4) is, despite the high similarities between hDPP4 and mDPP4 receptors. The variability of DPP4 receptors against MERS-CoV is not fully investigated, especially conformational and structural differences. Therefore, investigating the conformational differences of the DPP4 receptors can aid in developing new small animal models for MERS-CoV vaccines and antiviral agents evaluation. Here we used MD simulations and docking techniques to investigate these structural differences in DPP4 receptors. The results showed chimeric mouse mDPP4 (cmDPP4) has a similar compact conformation as wild-type hDPP4 based on the structural analysis. Interestingly, a single Thr288Ala mutation induced a relaxed conformation in chimeric 2 hDPP4 (c2hDPP4) and chimeric 2 mDPP4 (c2mDPP4); in addition to its significant effect on the DPP4 flexibility. The Thr288 residue is known for its critical function in MERS-CoV RBD interaction. Moreover, MERS-CoV RBD adopts a "standing" conformation when docked to hDPP4 and cmDPP4 in blade IV and V regions. In conclusion, the results could explain the functionality differences between mouse and human DPP4 receptors against MERS-CoV. However, further structural studies are needed to evaluate how DPP4 conformations affects MERS-CoV RBD binding and affinity.Communicated by Ramaswamy H. Sarma.
  • |*Middle East Respiratory Syndrome Coronavirus/genetics[MESH]
  • |Animals[MESH]
  • |Dipeptidyl Peptidase 4/genetics[MESH]


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